Literature DB >> 19218339

Identification of potential therapeutic targets in malignant mesothelioma using cell-cycle gene expression analysis.

Solange Romagnoli1, Ester Fasoli, Valentina Vaira, Monica Falleni, Caterina Pellegrini, Anna Catania, Massimo Roncalli, Antonio Marchetti, Luigi Santambrogio, Guido Coggi, Silvano Bosari.   

Abstract

Cell-cycle defects are responsible for cancer onset and growth. We studied the expression profile of 60 genes involved in cell cycle in a series of malignant mesotheliomas (MMs), normal pleural tissues, and MM cell cultures using a quantitative polymerase chain reaction-based, low-density array. Nine genes were significantly deregulated in MMs compared with normal controls. Seven genes were overexpressed in MMs, including the following: CDKN2C, cdc6, cyclin H, cyclin B1, CDC2, FoxM1, and Chk1, whereas Ube1L and cyclin D2 were underexpressed. Chk1 is a principal mediator of cell-cycle checkpoints in response to genotoxic stress. We confirmed the overexpression of Chk1 in an independent set of 87 MMs by immunohistochemistry using tissue microarrays. To determine whether Chk1 down-regulation would affect cell-cycle control and cell survival, we transfected either control or Chk1 siRNA into two mesothelioma cell lines and a nontumorigenic (Met5a) cell line. Results showed that Chk1 knockdown increased the apoptotic fraction of MM cells and induced an S phase block in Met5a cells. Furthermore, Chk1 silencing sensitized p53-null MM cells to both an S phase block and apoptosis in the presence of doxorubicin. Our results indicate that cell-cycle gene expression analysis by quantitative polymerase chain reaction can identify potential targets for novel therapies. Chk1 knockdown could provide a novel therapeutic approach to arrest cell-cycle progression in MM cells, thus increasing the rate of cell death.

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Year:  2009        PMID: 19218339      PMCID: PMC2665738          DOI: 10.2353/ajpath.2009.080721

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  50 in total

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3.  Control of cell cycle progression in human mesothelioma cells treated with gamma interferon.

Authors:  C Vivo; F Lévy; Y Pilatte; J Fleury-Feith; P Chrétien; I Monnet; L Kheuang; M C Jaurand
Journal:  Oncogene       Date:  2001-03-01       Impact factor: 9.867

4.  p27 immunostaining is related to prognosis in malignant mesothelioma.

Authors:  T W Beer; P Shepherd; N C Pullinger
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5.  Gene expression profiling of malignant mesothelioma.

Authors:  Sunil Singhal; Rainer Wiewrodt; Liliana D Malden; Kunjlata M Amin; Kimberly Matzie; Joseph Friedberg; John C Kucharczuk; Leslie A Litzky; Steven W Johnson; Larry R Kaiser; Steven M Albelda
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6.  Autocrine inhibitory influences of alpha-melanocyte-stimulating hormone in malignant pleural mesothelioma.

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9.  Inactivation of p16INK4a expression in malignant mesothelioma by methylation.

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  19 in total

Review 1.  Overexpressed genes in malignant pleural mesothelioma: implications in clinical management.

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2.  Nucleophosmin interacts with FOXM1 and modulates the level and localization of FOXM1 in human cancer cells.

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4.  Abrogating G₂/M checkpoint through WEE1 inhibition in combination with chemotherapy as a promising therapeutic approach for mesothelioma.

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5.  Spontaneous mesotheliomas in F344/N rats are characterized by dysregulation of cellular growth and immune function pathways.

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Review 6.  A new target for proteasome inhibitors: FoxM1.

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7.  Apoptosis induced by piroxicam plus cisplatin combined treatment is triggered by p21 in mesothelioma.

Authors:  Alfonso Baldi; Maria Teresa Piccolo; Maria Rosaria Boccellino; Aldo Donizetti; Irene Cardillo; Raffaele La Porta; Lucio Quagliuolo; Enrico P Spugnini; Francesca Cordero; Gennaro Citro; Massimo Menegozzo; Raffaele A Calogero; Stefania Crispi
Journal:  PLoS One       Date:  2011-08-17       Impact factor: 3.240

8.  miR-296 regulation of a cell polarity-cell plasticity module controls tumor progression.

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9.  Molecular resistance fingerprint of pemetrexed and platinum in a long-term survivor of mesothelioma.

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10.  An RNAi-based screen reveals PLK1, CDK1 and NDC80 as potential therapeutic targets in malignant pleural mesothelioma.

Authors:  A Linton; Y Y Cheng; K Griggs; Lyn Schedlich; M B Kirschner; S Gattani; S Srikaran; S Chuan-Hao Kao; B C McCaughan; S Klebe; N van Zandwijk; G Reid
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